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Noncytotoxic functions of killer cell granzymes in viral infections

Lisanne C. de Jong, Sandra Crnko, Toine ten Broeke, Niels Bovenschen

2021PLoS Pathogens30 citationsDOIOpen Access PDF

Abstract

Cytotoxic lymphocytes produce granules armed with a set of 5 serine proteases (granzymes (Gzms)), which, together with the pore-forming protein (perforin), serve as a major defense against viral infections in humans. This granule-exocytosis pathway subsumes a well-established mechanism in which target cell death is induced upon perforin-mediated entry of Gzms and subsequent activation of various (apoptosis) pathways. In the past decade, however, a growing body of evidence demonstrated that Gzms also inhibit viral replication and potential reactivation in cell death-independent manners. For example, Gzms can induce proteolysis of viral or host cell proteins necessary for the viral entry, release, or intracellular trafficking, as well as augment pro-inflammatory antiviral cytokine response. In this review, we summarize current evidence for the noncytotoxic mechanisms and roles by which killer cells can use Gzms to combat viral infections, and we discuss the potential thereof for the development of novel therapies.

Topics & Concepts

GranzymePerforinProteasesBiologyProgrammed cell deathExocytosisGranulysinCell biologyCytotoxic T cellImmunologyApoptosisImmune systemSecretionCD8EnzymeBiochemistryIn vitroImmune Cell Function and InteractionAutoimmune and Inflammatory Disorders ResearchMosquito-borne diseases and control
Noncytotoxic functions of killer cell granzymes in viral infections | Litcius